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垂体腺苷酸环化酶激活多肽38对生长激素和催乳素表达的影响。

Effect of pituitary adenylate cyclase-activating polypeptide 38 on growth hormone and prolactin expression.

作者信息

Velkeniers B, Zheng L, Kazemzadeh M, Robberecht P, Vanhaelst L, Hooghe-Peters E L

机构信息

Department of Pharmacology, Medical School, Vrije Universiteit Brussel, Belgium.

出版信息

J Endocrinol. 1994 Oct;143(1):1-11. doi: 10.1677/joe.0.1430001.

Abstract

Time- and dose-dependent effects of pituitary adenylate cyclase-activating polypeptide (PACAP) on prolactin (PRL) and growth hormone (GH) release were examined in static and dynamic rat pituitary cell incubations and on different pituitary cell (sub)populations separated according to their density on a discontinuous Percoll gradient. Quantitative in situ hybridization histochemistry allowed us to examine in parallel the effects of PACAP on PRL and GH gene expression. PACAP did not alter GH or PRL secretion in a dynamic superfusion system, in any cell population tested. Static incubations (30 min, 2-36 h) with PACAP 38 resulted in a significant increase in GH release and stimulated GH synthesis, as measured by the cytoplasmic accumulation of GH mRNA in the somatotrophs. These effects on synthesis and release were also observed after the enrichment of GH cells on Percoll gradients. PRL release was not altered by longer periods of incubation. Although no significant changes were observed in PRL secretion after 38 h, accumulation of cytoplasmic PRL mRNA was significantly stimulated in total pituitary cell suspension. After fractioning lactotrophs on Percoll gradients, the stimulatory effect of PACAP on PRL synthesis was lost. These results suggest that PACAP stimulates GH release and synthesis, and that it may act as a physiological regulator of this cell type. The PRL cell is not the most likely target cell type for PACAP. Effects observed on PRL synthesis in the total cell population may involve paracrine action of other hormone- or non-hormone-secreting cell types.

摘要

在静态和动态大鼠垂体细胞培养以及根据不连续Percoll梯度上的密度分离的不同垂体细胞(亚)群体中,研究了垂体腺苷酸环化酶激活多肽(PACAP)对催乳素(PRL)和生长激素(GH)释放的时间和剂量依赖性影响。定量原位杂交组织化学使我们能够同时研究PACAP对PRL和GH基因表达的影响。在任何测试的细胞群体中,PACAP在动态超灌注系统中均未改变GH或PRL的分泌。用PACAP 38进行静态孵育(30分钟,2 - 36小时)导致GH释放显著增加,并刺激了GH合成,这通过生长激素细胞中GH mRNA的细胞质积累来衡量。在Percoll梯度上富集GH细胞后,也观察到了对合成和释放的这些影响。较长时间的孵育并未改变PRL的释放。尽管在38小时后PRL分泌未观察到显著变化,但在全垂体细胞悬液中细胞质PRL mRNA的积累受到显著刺激。在Percoll梯度上对催乳素细胞进行分级分离后,PACAP对PRL合成的刺激作用消失。这些结果表明,PACAP刺激GH的释放和合成,并且它可能作为这种细胞类型的生理调节剂。PRL细胞不是PACAP最可能的靶细胞类型。在全细胞群体中观察到的对PRL合成的影响可能涉及其他激素分泌或非激素分泌细胞类型的旁分泌作用。

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